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肝移植耐受及其临床应用:我们能否利用高剂量效应?

Liver transplant tolerance and its application to the clinic: can we exploit the high dose effect?

作者信息

Cunningham Eithne C, Sharland Alexandra F, Bishop G Alex

机构信息

Collaborative Transplantation Research Group, Bosch Institute, Royal Prince Alfred Hospital and University of Sydney, Sydney, NSW 2006, Australia.

出版信息

Clin Dev Immunol. 2013;2013:419692. doi: 10.1155/2013/419692. Epub 2013 Nov 6.

Abstract

The tolerogenic properties of the liver have long been recognised, especially in regard to transplantation. Spontaneous acceptance of liver grafts occurs in a number of experimental models and also in a proportion of clinical transplant recipients. Liver graft acceptance results from donor antigen-specific tolerance, demonstrated by the extension of tolerance to other grafts of donor origin. A number of factors have been proposed to be involved in liver transplant tolerance induction, including the release of soluble major histocompatibility (MHC) molecules from the liver, its complement of immunosuppressive donor leucocytes, and the ability of hepatocytes to directly interact with and destroy antigen-specific T cells. The large tissue mass of the liver has also been suggested to act as a cytokine sink, with the potential to exhaust the immune response. In this review, we outline the growing body of evidence, from experimental models and clinical transplantation, which supports a role for large tissue mass and high antigen dose in the induction of tolerance. We also discuss a novel gene therapy approach to exploit this dose effect and induce antigen-specific tolerance robust enough to overcome a primed T cell memory response.

摘要

肝脏的致耐受性特性早已为人所知,尤其是在移植方面。在许多实验模型以及部分临床移植受者中,肝脏移植物可自发被接受。肝脏移植物的接受源于供体抗原特异性耐受,这通过对源自供体的其他移植物的耐受性扩展得以证明。人们提出了多种因素参与肝脏移植耐受的诱导,包括肝脏中可溶性主要组织相容性复合体(MHC)分子的释放、其免疫抑制性供体白细胞的组成成分,以及肝细胞直接与抗原特异性T细胞相互作用并将其破坏的能力。肝脏的巨大组织量也被认为可充当细胞因子库,有可能耗尽免疫反应。在本综述中,我们概述了来自实验模型和临床移植的越来越多的证据,这些证据支持大组织量和高抗原剂量在耐受诱导中的作用。我们还讨论了一种新型基因治疗方法,以利用这种剂量效应并诱导足够强大的抗原特异性耐受,从而克服已致敏的T细胞记忆反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a7cc/3836300/13318e92c8f7/CDI2013-419692.001.jpg

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